DNA damage and repair in Alzheimer's disease

The vast majority of the studies performed so far and aimed at elucidating DNA repair mechanisms has been performed in mitotic cells, such as transformed or cancer cell lines. Therefore, our understanding of DNA repair mechanisms in post-mitotic cells, such as neurons, remains one of the most exciti...

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Bibliographic Details
Published inCurrent Alzheimer research Vol. 6; no. 1; p. 36
Main Authors Coppedè, Fabio, Migliore, Lucia
Format Journal Article
LanguageEnglish
Published United Arab Emirates 01.02.2009
Subjects
Alzheimer Disease - genetics
Alzheimer Disease - metabolism
Alzheimer Disease - physiopathology
Animals
Cell Death - genetics
Cell Nucleus - genetics
Cell Nucleus - pathology
DNA Damage - genetics
DNA Repair - genetics
Genetic Predisposition to Disease - genetics
Humans
Nerve Degeneration - genetics
Nerve Degeneration - metabolism
Nerve Degeneration - physiopathology
Oxidative Stress - genetics
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Summary:The vast majority of the studies performed so far and aimed at elucidating DNA repair mechanisms has been performed in mitotic cells, such as transformed or cancer cell lines. Therefore, our understanding of DNA repair mechanisms in post-mitotic cells, such as neurons, remains one of the most exciting areas for future investigations. Markers of DNA damage, particularly oxidative DNA damage, have been largely found in brain regions, peripheral tissues, and biological fluids of Alzheimer's disease (AD) patients. Moreover, recent studies from our and other groups in individuals affected by Mild Cognitive Impairment provided evidence that oxidative DNA damage is one of the earliest detectable events within the progression from a normal brain to dementia. Almost one decade ago a decrease in the DNA base excision repair (BER) activity was observed in post mortem brain regions of AD individuals, leading to the hypothesis that the brain in AD might be subjected to the double insult of increased DNA damage, as well as deficiencies of DNA repair pathways. Subsequent studies have provided accumulating evidence of impaired DNA repair in AD. Moreover, functional variants and polymorphisms of DNA repair genes have been the focus of several cancer association studies, but only in recent years some of them have been investigated as possible AD risk factors. The few studies performed so far suggest that some variants might play a role in AD pathogenesis and deserve further investigations. Here, we summarize the current knowledge of DNA damage and repair in AD pathogenesis.
ISSN:1875-5828
DOI:10.2174/156720509787313970